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Publication : DNGR-1(+) dendritic cells are located in meningeal membrane and choroid plexus of the noninjured brain.

First Author  Quintana E Year  2015
Journal  Glia Volume  63
Issue  12 Pages  2231-48
PubMed ID  26184558 Mgi Jnum  J:225901
Mgi Id  MGI:5694888 Doi  10.1002/glia.22889
Citation  Quintana E, et al. (2015) DNGR-1(+) dendritic cells are located in meningeal membrane and choroid plexus of the noninjured brain. Glia 63(12):2231-48
abstractText  The role and different origin of brain myeloid cells in the brain is central to understanding how the central nervous system (CNS) responds to injury. C-type lectin receptor family 9, member A (DNGR-1/CLEC9A) is a marker of specific DC subsets that share functional similarities, such as CD8alpha(+) DCs in lymphoid tissues and CD103(+) CD11b(low) DCs in peripheral tissues. Here, we analyzed the presence of DNGR-1 in DCs present in the mouse brain (bDCs). Dngr-1/Clec9a mRNA is expressed mainly in the meningeal membranes and choroid plexus (m/Ch), and its expression is enhanced by fms-like tyrosine kinase 3 ligand (Flt3L), a cytokine involved in DC homeostasis. Using Clec9a(egfp/egfp) mice, we show that Flt3L induces accumulation of DNGR-1-EGFP(+) cells in the brain m/Ch. Most of these cells also express major histocompatibility complex class II (MHCII) molecules. We also observed an increase in specific markers of cDC CD8alpha+ cells such as Batf-3 and Irf-8, but not of costimulatory molecules such as Cd80 and Cd86, indicating an immature phenotype for these bDCs in the noninjured brain. The presence of DNGR-1 in the brain provides a potential marker for the study of this specific brain cell subset. Knowledge and targeting of brain antigen presenting cells (APCs) has implications for the fight against brain diseases such as neuroinflammation-based neurodegenerative diseases, microbe-induced encephalitis, and brain tumors such as gliomas. GLIA 2015;63:2231-2248.
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